Comparison of Phenotype in Uniparental Disomy and Deletion Prader-Willi Syndrome: Sex Specific Differences

Overview

Journal Am J Med Genet

Specialty Genetics

Date 1996 Oct 16

PMID 8911605

Citations 12

Authors

J Mitchell

A Schinzel

S Langlois

G Gillessen-Kaesbach

S Schuffenhauer

R Michaelis

D Abeliovich

I Lerer

S Christian

M Guitart

D E McFadden

W P Robinson

Affiliations

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Abstract

Prader-Willi syndrome (PWS) results primarily from either a paternal deletion of 15q11-q13 or maternal uniparental disomy (UPD) 15. Birth parameters and clinical presentation of 79 confirmed UPD cases and 43 deletion patients were compared in order to test whether any manifestations differ between the two groups. There were no major clinical differences between the two classes analyzed as a whole, other than the presence of hypopigmentation predominantly in the deletion group. However, there was a significant bias in sex-ratio (P < .001) limited to the UPD group with a predominance (68%) of males. An equal number of males and females was observed in the deletion group. When analyzed by sex, several significant differences between the UPD and deletion groups were observed. Female UPD patients were found to be less severely affected than female deletion patients in terms of length of gavage feeding and a later onset of hyperphagia. Although these traits are likely to be influenced by external factors, they may reflect a milder presentation of female UPD patients which could explain the observed sex bias by causing under-ascertainment of female UPD. Alternatively, there may be an effect of sex on either early trisomy 15 survival or the probability of somatic loss of a chromosome from a trisomic conceptus.

Citing Articles

Copy neutral absence of heterozygosity on chromosome 15 distal long arm: A surrogate marker for Prader-Willi/Angelman syndromes?.

Ortega V, Louie R, Jones M, Chaubey A, DuPont B, Britt A Mol Cytogenet. 2021; 14(1):37.

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Comprehensive meta-analysis reveals association between multiple imprinting disorders and conception by assisted reproductive technology.

Cortessis V, Azadian M, Buxbaum J, Sanogo F, Song A, Sriprasert I J Assist Reprod Genet. 2018; 35(6):943-952.

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Does the Genetic Cause of Prader-Willi Syndrome Explain the Highly Variable Phenotype?.

Dobrescu A, Chirita-Emandi A, Andreescu N, Farcas S, Puiu M Maedica (Bucur). 2017; 11(3):191-197.

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Prader-Willi Syndrome: Clinical and Genetic Findings.

Butler M, Thompson T Endocrinologist. 2016; 10(4 Suppl 1):3S-16S.

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Gender Differences in the Behavioral Symptom Severity of Prader-Willi Syndrome.

Gito M, Ihara H, Ogata H, Sayama M, Murakami N, Nagai T Behav Neurol. 2015; 2015:294127.

PMID: 26633919 PMC: 4655018. DOI: 10.1155/2015/294127.